A genetically adjuvanted influenza B virus vector increases immunogenicity and protective efficacy in mice

被引:0
|
作者
Christian Kittel
Nina Wressnigg
Anna Polina Shurygina
Markus Wolschek
Marina Stukova
Ekatherina Romanovskaya-Romanko
Julia Romanova
Oleg Kiselev
Thomas Muster
Andrej Egorov
机构
[1] Avir Green Hills Biotechnology AG,Influenza Research Institute
[2] Russian Academy of Medical Sciences,undefined
来源
Archives of Virology | 2015年 / 160卷
关键词
Influenza; Virus Vector; Vero Cell; Influenza Vaccine; Hemagglutination Inhibition;
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学科分类号
摘要
The existence of multiple antigenically distinct types and subtypes of influenza viruses allows the construction of a multivalent vector system for the mucosal delivery of foreign sequences. Influenza A viruses have been exploited successfully for the expression of extraneous antigens as well as immunostimulatory molecules. In this study, we describe the development of an influenza B virus vector whose functional part of the interferon antagonist NS1 was replaced by human interleukin 2 (IL2) as a genetic adjuvant. We demonstrate that IL2 expressed by this viral vector displays immune adjuvant activity in immunized mice. Animals vaccinated with the IL2 viral vector showed an increased hemagglutination inhibition antibody response and higher protective efficacy after challenge with a wild-type influenza B virus when compared to mice vaccinated with a control virus. Our results demonstrate that it is feasible to construct influenza B vaccine strains expressing immune-potentiating foreign sequences from the NS genomic segment. Based on these data, it is now hypothetically possible to create a trivalent (or quadrivalent) live attenuated influenza vaccine in which each component expresses a selected genetic adjuvant with tailored expression levels.
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页码:2525 / 2534
页数:9
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